Novel ATRX gene damaging missense mutation c.6740A>C segregates with profound to severe intellectual deficiency without alpha thalassaemia.

Bouazzi, Habib; Thakur, Seema; Trujillo, Carlos; Alwasiyah, Mohammad Khalid; Munnich, Arnold

Novel ATRX gene damaging missense mutation c.6740A>C segregates with profound to severe intellectual deficiency without alpha thalassaemia.

Files

ijmr2016v143n1p43.pdf (1.57 MB)

Date

2016-01

Authors

Bouazzi, Habib

Thakur, Seema

Trujillo, Carlos

Alwasiyah, Mohammad Khalid

Munnich, Arnold

Abstract

Background & objectives: ATRX is a recessive X-linked intellectual deficiency (X-LID) gene causing predominately alpha-thalassaemia with a wide and clinically heterogeneous spectrum of intellectual deficiency syndromes. Although alpha-thalassaemia is commonly present, some patients do not express this sign despite the ATRX gene being altered. Most pathological mutations have been localized in two different major domains, the helicase and the plant homeo-domain (PHD)-like domain. In this study we examined a family of three males having an X-linked mental deficiency and developmental delay, and tried to establish a genetic diagnosis while discussing and comparing the phenotype of our patients to those reported in the literature. Methods: Three related males with intellectual deficiency underwent clinical investigations. We performed a karyotype analysis, CGH-array, linkage study, and X-exome sequencing in the index case to identify the genetic origin of this disorder. The X-inactivation study was carried out in the mother and Sanger sequencing was achieved in all family members to confirm the mutation. Results: A novel ATRX gene missense mutation (p.His2247Pro) was identified in a family of two uncles and their nephew manifesting intellectual deficiency and specific facial features without alpha-thalassaemia. The mutation was confirmed by Sanger sequencing. It segregated with the pathological phenotype. The mother and her two daughters were found to be heterozygous. Interpretation & conclusions: The novel mutation c.6740A>C was identified within the ATRX gene helicase domain and confirmed by Sanger sequencing in the three affected males as well as in the mother and her two daughters. This mutation was predicted to be damaging and deleterious. The novel mutation segregated with the phenotype without alpha-thalassaemia and with non-skewed X chromosome.

Keywords

Alpha thalassaemia, ATRX - exome sequencing, intellectual deficiency, novel mutation, X inactivation

Citation

Bouazzi Habib, Thakur Seema, Trujillo Carlos, Alwasiyah Mohammad Khalid, Munnich Arnold. Novel ATRX gene damaging missense mutation c.6740A>C segregates with profound to severe intellectual deficiency without alpha thalassaemia. Indian Journal of Medical Research. 2016 Jan; 143(1): 43-48.

URI

https://imsear.searo.who.int/handle/123456789/176409

Collections

Indian Journal of Medical Research

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